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Hemoglobin
international journal for hemoglobin research
Volume 32, 2008 - Issue 5
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Original Article

Molecular Basis of Thalassemia Intermedia in Iran

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Pages 462-470 | Received 25 Dec 2007, Accepted 19 Mar 2008, Published online: 07 Jul 2009
 

Abstract

Thalassemia intermedia shows considerable heterogenity in phenotype and molecular basis. The aim of this study was to evaluate the prevalence and effect of different β-globin mutations, α-globin defects and Gγ XmnI polymorphisms in Iranian patients. Forty-five Iranian patients with clinical criteria of thalassemia intermedia were studied. The molecular background of the diseases was investigated. The mean age of onset varied from 1.5 to 30 years. Only 22.2% of cases received occasional blood transfusions. The hemoglobin (Hb) level in more than half of the cases was stable (10–12 g/dL) with no need for blood transfusions. In most cases (88.9%) the Hb F level was more than 50%. Sixty-eight point nine percent of patients were homozygous for β0-thalassemia (β-thal) mutations. The positive XmnI polymorphism with the capability of enhancing Hb F production was seen in 60% of the studied chromosomes. Co-inheritance of α-globin gene defects was seen in 22.2% of cases. Only 8.9% of patients had β+ or β++ mutations.

We concluded that the main molecular basis of the thalassemia intermedia phenotype in Iranian cases is co-inheritance of a positive XmnI polymorphism with β-globin mutations, which can enhance the capability of Hb F production. Co-inheritance of α-globin defects and mild β-globin mutations are second and third causes of thalassemia intermedia phenotypes respectively. These factors must be considered in genetic counseling, prediction of disease prognosis and treatment and prenatal diagnosis.

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